A team of scientists at VCU Massey Comprehensive Cancer Center have successfully developed a groundbreaking targeted therapy that hones in on the KRAS protein.
The KRAS protein drives some of the deadliest human cancers, including pancreatic, lung and colon tumors. Their findings are published in Cancer Research Communications.
Through a highly collaborative research effort led by the laboratory of Dr. Saïd Sebti at the VCU Massey Comprehensive Cancer Center, a team of scientists suggest that a novel inhibitor drug could be used to target KRAS G12D, a subset of the notorious cancer-driving KRAS gene. The research involved the combined efforts of scientists from multiple esteemed cancer centers, including three National Cancer Institute-designated cancer centers, Moffitt Cancer Center, Montefiore Einstein Comprehensive Cancer Center, University of Florida Health Cancer Center, and the Cancer Center at Illinois.
“This discovery is a major step forward in our battle against some of the most aggressive forms of cancer,” said Sebti, the associate director for basic research and the Lacy Family Chair in Cancer Research at Massey. “Our collaborative effort signifies a leap forward in the development of targeted therapies against KRAS-driven cancers such as pancreatic cancer.”
Sebti’s team screened a library of compounds in partnership with the Cancer Center at Illinois to identify drugs that attach themselves to KRAS and thwart it, preventing it from causing cancer. The most potent drug they identified through this process, KRAS Binder-456 (KRB-456), was then evaluated by Sebti and his team to understand its biological mechanism of action. They demonstrated that KRB-456 significantly inhibits the growth in mice of mutant KRAS-addicted tumors derived from pancreatic cancer patients who had not responded to, or relapsed following, traditional chemotherapy or radiation therapy.
Further investigation is planned, according to Sebti, to test the drug in combination with standard-of-care therapeutic options to explore its potential as an effective supplement to cancer treatment, or to possibly inform the development of a more potent or selective drug against KRAS G12D-driven tumors.
“For every researcher in the field of oncology, the ultimate aspiration is to make a tangible difference in the lives of cancer patients. As we progress toward this goal, the excitement mounts, knowing that our work could directly impact those battling this devastating disease,” said Sebti, who is also a professor in the Department of Pharmacology and Toxicology at the VCU School of Medicine. “KRAS used to be called the ‘undruggable target.’ But we and others have now shown that it is druggable. We’re hoping that our continued work will lead to the development of effective drugs for KRAS G12D-driven cancers.”
More than 90 percent of pancreatic cancers, about 35 percent of colon tumors and roughly one-quarter of lung tumors have a mutant KRAS gene, Sebti said.
“It’s about targeting the mutation, not necessarily the disease,” Sebti said. “We anticipate that our findings will help identify a therapeutic option that would also work for lung and colon tumors that also have this specific KRAS G12D mutation.”
The new research discovery builds on nearly a decade’s worth of research led by Sebti at different cancer centers investigating the KRAS gene’s involvement in cancer development.
Sebti’s laboratory at Massey, one of only two NCI-designated cancer centers in Virginia, is dedicated to research in cancer biology and therapeutic interventions. Through innovative collaborations and cutting-edge technology, the lab strives to unravel the complexities of cancer and develop novel strategies for effective treatment of disease.
The research work was funded by multiple grants from the National Institutes of Health/National Cancer Institute and, in part, by Massey’s Cancer Center Support Grant.
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Rebecca Barnabi
